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采用电喷雾(ESI)正离子模式和正离子光电离(PSI)模式探索设计药物的化学特征-关于碎裂机制和化学计量学分析的方法。

Exploring the chemical profile of designer drugs by ESI(+) and PSI(+) mass spectrometry-An approach on the fragmentation mechanisms and chemometric analysis.

机构信息

Laboratório de Petroleômica e Forense, Universidade Federal do Espírito Santo (UFES), Avenida Fernando Ferrari, 514, Goiabeiras, Vitória, ES, CEP: 29075-910, Brazil.

Instituto Nacional de Ciência e Tecnologia Forense (INCT Forense), Vitoria, Brazil.

出版信息

J Mass Spectrom. 2020 Oct;55(10):e4596. doi: 10.1002/jms.4596.

DOI:10.1002/jms.4596
PMID:32729201
Abstract

The consumption of design drugs, frequently known as new psychoactive substances (NPS), has increased considerably worldwide, becoming a severe issue for the responsible governmental agencies. These illicit substances can be defined as synthetic compounds produced in clandestine laboratories in order to act as analogs of schedule drugs mimetizing its chemical structure and improving its pharmacological effects while hampering the control and making regulation more complicated. In this way, the development of new methodologies for chemical analysis of NPS drugs is indispensable to determine a novel class of drugs arising from the underground market. Therefore, this work shows the use of high-resolution mass spectrometry Fourier transform ion cyclotron resonance mass spectrometry (FT-ICR MS) applying different ionization sources such as paper spray ionization (PSI) and electrospray ionization (ESI) in the evaluation of miscellaneous of seized drugs samples as blotter paper (n = 79) and tablet (n = 100). Also, an elucidative analysis was performed by ESI(+)MS/MS experiments, and fragmentation mechanisms were proposed to confirm the chemical structure of compounds identified. Besides, the results of ESI(+) and PSI(+)-FT-ICR MS were compared with those of GC-MS, revealing that ESI(+)MS showed greater detection efficiency among the methodologies employed in this study. Moreover, this study stands out as a guide for the chemical analysis of NPS drugs, highlighting the differences between the techniques of ESI(+)-FT-ICR MS, PSI(+)-FT-ICR MS, and GC-MS.

摘要

新精神活性物质(NPS)在世界范围内的消费大幅增加,成为负责政府机构的一个严重问题。这些非法物质可以被定义为在秘密实验室中生产的合成化合物,目的是作为管制药物的类似物,模拟其化学结构并提高其药理作用,同时阻碍管制并使法规更加复杂。因此,开发用于 NPS 药物化学分析的新方法学对于确定源自地下市场的新型药物类别是不可或缺的。因此,这项工作展示了使用高分辨率质谱傅里叶变换离子回旋共振质谱(FT-ICR MS),应用不同的离子源,如纸喷雾电离(PSI)和电喷雾电离(ESI),对各种缴获的药物样本进行评估,包括纸条(n=79)和片剂(n=100)。此外,还通过 ESI(+)MS/MS 实验进行了阐明性分析,并提出了碎裂机制来确认鉴定化合物的化学结构。此外,ESI(+)和 PSI(+) - FT-ICR MS 的结果与 GC-MS 的结果进行了比较,结果表明 ESI(+)MS 在本研究中使用的方法学中具有更高的检测效率。此外,这项研究为 NPS 药物的化学分析提供了指导,突出了 ESI(+) - FT-ICR MS、PSI(+) - FT-ICR MS 和 GC-MS 技术之间的差异。

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